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大麻二酚二醇,一种来自大麻的二聚植物大麻素,是一种选择性的热 TRP 调节剂。

Cannabitwinol, a Dimeric Phytocannabinoid from Hemp, L., Is a Selective Thermo-TRP Modulator.

机构信息

Department of Pharmacy, School of Medicine and Surgery, University of Naples Federico II, Via D. Montesano 49, 80131 Napoli, Italy.

Endocannabinoid Research Group (ERG)-Institute of Biomolecular Chemistry (ICB)-National Research Council (CNR), Via Campi Flegrei 34, 80078 Pozzuoli (NA), Italy.

出版信息

J Nat Prod. 2020 Sep 25;83(9):2727-2736. doi: 10.1021/acs.jnatprod.0c00668. Epub 2020 Sep 3.

Abstract

Cannabitwinol (CBDD, ), the second member of a new class of dimeric phytocannabinoids in which two units are connected by a methylene bridge, was isolated from a hemp ( L.) industrial extract. The structural characterization of cannabitwinol, complicated by broadening of H NMR signals and lack of expected 2D NMR correlations at room temperature, was fully carried out in methanol- at -30 °C. All the attempts to prepare CBDD by reaction of CBD with formaldehyde or its iminium analogue (Eschenmoser salt) failed, suggesting that this sterically congested dimer is the result of enzymatic reactions on the corresponding monomeric acids. Analysis of the cannabitwinol profile of transient receptor potential (TRP) modulation evidenced the impact of dimerization, revealing a selectivity for channels activated by a decrease of temperature (TRPM8 and TRPA1) and the lack of significant affinity for those activated by an increase of temperature (e.g., TRPV1). The putative binding modes of cannabitwinol with TRPA1 and TRPM8 were investigated in detail by a molecular docking study using the homology models of both channels.

摘要

大麻二酚二聚体(CBDD,)是一类新型二聚体植物大麻素中的第二个成员,两个单元通过亚甲基桥连接。它是从大麻(L.)工业提取物中分离出来的。由于大麻二酚二聚体的核磁共振信号变宽,且在室温下缺乏预期的二维核磁共振相关信号,其结构特征的全面表征非常复杂。在甲醇-30°C 下,对大麻二酚二聚体进行了全面的结构表征。所有试图通过 CBD 与甲醛或其亚胺类似物(Eschenmoser 盐)反应制备 CBDD 的尝试都失败了,这表明这种空间位阻拥挤的二聚体是相应单体酸的酶促反应的结果。对瞬时受体电位(TRP)调制的大麻二酚二聚体谱分析证明了二聚化的影响,揭示了其对温度下降激活的通道(TRPM8 和 TRPA1)的选择性,以及对温度升高激活的通道(如 TRPV1)缺乏显著亲和力。通过使用两种通道的同源模型,进行分子对接研究,详细研究了大麻二酚二聚体与 TRPA1 和 TRPM8 的可能结合模式。

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